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Nical assistance.Author ContributionsConceived and designed the experiments: MG NF LM

Published August 24, 2017 by MEK Inhibitor- sgkinhibitor

Nical assistance.Author ContributionsConceived and designed the experiments: MG NF LM ALGV. Performed the experiments: MG JCF GCT SA ALGV. Analyzed the data: MG ALGV. Contributed reagents/materials/analysis tools: NF LM. Wrote the paper: MG ALGV.Effects of Ischemia in Early OvernutritionPyruvate carboxylase (PC) is an important anaplerotic enzyme that catalyzes the ATP-driven carboxylation of pyruvate to oxaloaceate. This reaction is not only the first important committed step of hepatic gluconeogenesis but also crucial for cataplerosis as Krebs cycle intermediates are withdrawn for AZ-876 various biosynthetic purposes including de novo fatty acid synthesis in liver and adipose tissue, glyceroneogenesis in adipose tissue and glutamate production in astrocytes (for review see [1?]). PC also plays an important role in normal glucose-stimulated insulin secretion (GSIS) in pancreatic b-cells [4?]. Dysregulation of PC expression in liver, adipose tissue or islets is also associated with obesity and type 2 diabetes [7?1]. PC deficiency is a rare autosomal recessive phenotype characterized by mild to severe lactic acidemia associated with delayed psychomotor development and death within the first year of life in about one-half the cases [12]. PC is allosterically activated by acetyl-CoA, a signaling molecule that is produced by increased fatty acid oxidation during prolonged starvation. In mammals, the PC gene is transcriptionally regulated by alternate promoters which mediate the production of multiple mRNA isoforms which differ in their 59-untranslated regions. The PC genes from rat and mouse arewell characterized and they are controlled by two promoters namely the proximal and the distal promoters [13?5]. The proximal promoter is responsible for production of PC mRNA in the gluconeogenic tissues including liver and kidney, as well as the lipogenic tissues including liver and adipose tissues. The presence of a cAMP-responsive element (CRE) [16]) and a peroxisome proliferator activated receptor response element (PPRE) [17] in the proximal promoter allows liver and adipose tissue, respectively, to produce more PC during prolonged fasting. In contrast, the distal promoter is linked to anaplerosis especially in pancreatic b-cells. The structural region of the human PC gene has been cloned and characterized [18]. However, the regulatory regions of the PC gene that confer tissue-specific expression of PC in humans are not known. Recently, Wang et al [19] reported that unlike the rat and mouse PC genes, the human PC gene is transcribed from three promoters. Herein, we present evidence that similar to the rodent PC genes, the human PC gene is transcribed from two promoters. In addition, we identified some of the important cisacting elements of the distal human PC promoter that direct transcription of PC in beta cells.Distal Promoter of the Human Pyruvate CarboxylaseDistal Promoter of the Human Pyruvate CarboxylaseFigure 1. RT-PCR analysis of PC mRNA variants in human liver and human pancreatic islets. (A) Schematic diagram showing alignment of 3 variants of human PC mRNA (GenBank NM_000920.3, NM_022172.2, BC011617.2). (B) Schematic diagram showing the Pentagastrin structure of the human PC gene. Two isoforms of human PC mRNA are initiated by two alternative promoters, the proximal (P1) promoter and the distal (P2) promoter. All PC mRNA variants contain the same coding sequences but differ in their 59-untranslated regions (UTR) produced from different 59-UTR exons (UE1/.Nical assistance.Author ContributionsConceived and designed the experiments: MG NF LM ALGV. Performed the experiments: MG JCF GCT SA ALGV. Analyzed the data: MG ALGV. Contributed reagents/materials/analysis tools: NF LM. Wrote the paper: MG ALGV.Effects of Ischemia in Early OvernutritionPyruvate carboxylase (PC) is an important anaplerotic enzyme that catalyzes the ATP-driven carboxylation of pyruvate to oxaloaceate. This reaction is not only the first important committed step of hepatic gluconeogenesis but also crucial for cataplerosis as Krebs cycle intermediates are withdrawn for various biosynthetic purposes including de novo fatty acid synthesis in liver and adipose tissue, glyceroneogenesis in adipose tissue and glutamate production in astrocytes (for review see [1?]). PC also plays an important role in normal glucose-stimulated insulin secretion (GSIS) in pancreatic b-cells [4?]. Dysregulation of PC expression in liver, adipose tissue or islets is also associated with obesity and type 2 diabetes [7?1]. PC deficiency is a rare autosomal recessive phenotype characterized by mild to severe lactic acidemia associated with delayed psychomotor development and death within the first year of life in about one-half the cases [12]. PC is allosterically activated by acetyl-CoA, a signaling molecule that is produced by increased fatty acid oxidation during prolonged starvation. In mammals, the PC gene is transcriptionally regulated by alternate promoters which mediate the production of multiple mRNA isoforms which differ in their 59-untranslated regions. The PC genes from rat and mouse arewell characterized and they are controlled by two promoters namely the proximal and the distal promoters [13?5]. The proximal promoter is responsible for production of PC mRNA in the gluconeogenic tissues including liver and kidney, as well as the lipogenic tissues including liver and adipose tissues. The presence of a cAMP-responsive element (CRE) [16]) and a peroxisome proliferator activated receptor response element (PPRE) [17] in the proximal promoter allows liver and adipose tissue, respectively, to produce more PC during prolonged fasting. In contrast, the distal promoter is linked to anaplerosis especially in pancreatic b-cells. The structural region of the human PC gene has been cloned and characterized [18]. However, the regulatory regions of the PC gene that confer tissue-specific expression of PC in humans are not known. Recently, Wang et al [19] reported that unlike the rat and mouse PC genes, the human PC gene is transcribed from three promoters. Herein, we present evidence that similar to the rodent PC genes, the human PC gene is transcribed from two promoters. In addition, we identified some of the important cisacting elements of the distal human PC promoter that direct transcription of PC in beta cells.Distal Promoter of the Human Pyruvate CarboxylaseDistal Promoter of the Human Pyruvate CarboxylaseFigure 1. RT-PCR analysis of PC mRNA variants in human liver and human pancreatic islets. (A) Schematic diagram showing alignment of 3 variants of human PC mRNA (GenBank NM_000920.3, NM_022172.2, BC011617.2). (B) Schematic diagram showing the structure of the human PC gene. Two isoforms of human PC mRNA are initiated by two alternative promoters, the proximal (P1) promoter and the distal (P2) promoter. All PC mRNA variants contain the same coding sequences but differ in their 59-untranslated regions (UTR) produced from different 59-UTR exons (UE1/.